Greetings, and welcome to the Alkermes Second Quarter 2022 Earnings Call. My name is Melissa, and I will be your operator for today's call. All participant lines will be placed on mute to prevent any background noise. If you should require operator assistance during the conference, please press star zero on your telephone keypad. Please note that this conference is being recorded. I'll now turn the call over to Sandy Coombs, Senior Vice President of Investor Relations and Corporate Affairs. Sandy, you may begin.
Thank you. Good morning, and welcome to the Alkermes plc conference call to discuss our financial results and business update for the quarter ended June 30, 2022. With me today are Richard Pops, our CEO, Iain Brown, our CFO, and Todd Nichols, our Chief Commercial Officer. Before we begin, I encourage everyone to go to the investor section of alkermes.com to find our press release, related financial tables, and reconciliations of the GAAP to non-GAAP financial measures that we'll discuss today. We believe the non-GAAP financial results, in conjunction with the GAAP results, are useful in understanding the ongoing economics of our business. Our discussions during this conference call will include forward-looking statements. Actual results could differ materially from these forward-looking statements.
Please see slide two of the accompanying presentation, our press release issued this morning, and our most recent annual and quarterly reports filed with the SEC for important risk factors that could cause our actual results to differ materially from those expressed or implied in the forward-looking statements. We undertake no obligation to update or revise the information provided on this call or in the accompanying presentation as a result of new information or future results or developments. After our prepared remarks, we'll open the call for Q&A, and now I'll turn the call over to Iain.
Thank you, Sandy. Hello, everyone, and thank you for joining our call today. We delivered strong results during the second quarter, driven by the performance of our proprietary commercial products and our disciplined management of our cost structure. The launch of LYBALVI continued to perform well during the quarter, and we're pleased to raise our financial expectations for the year based on this performance and updated assumptions related to our royalties from sales of the long-acting Invega products outside the United States. These top-line improvements are expected to flow through to our bottom-line results for the year, and I'll provide additional detail on these expectations in a moment. First, I'll start with an overview of our second quarter financial highlights.
We generated total revenues of $276.2 million, driven by strength in our proprietary commercial product portfolio, which increased net sales by approximately 19% year-over-year. Starting with VIVITROL, net sales in the second quarter were $96.1 million, reflecting 9% growth year-over-year. Gross to net adjustments in the second quarter of 51.1% reflected continued favorability with respect to previously booked Medicaid reserves. In Q2, inventory in the channel decreased by approximately $1 million, consistent with typical seasonal and shipping patterns. Today, we are narrowing our expectation for VIVITROL net sales for the full year from a range of $355 million-$385 million to a range of $365 million-$385 million.
We now expect gross to net adjustments to be approximately 51% for the full year, revised from our previous expectation of 52%. The ARISTADA product family generated net sales of $74.6 million, a 3% increase year-over-year. Gross to net adjustments were 54.2% in the second quarter, and inventory levels decreased by approximately $2 million. Today, we're narrowing our ARISTADA net sales range for the full year from a range of $290 million-$320 million to a range of $295 million-$315 million. We continue to expect gross to net adjustments of approximately 54% for the full year.
Looking ahead to the third quarter, we expect growth of these two products to moderate consistent with typical seasonal patterns with more robust growth expected to resume in the fourth quarter. LYBALVI net sales in the second quarter increased 44% sequentially to $21 million, driven primarily by demand growth. In Q2, inventory levels increased by approximately $1.8 million in line with demand and gross to net adjustments in the quarter were 26%, primarily reflecting a continuation of less restrictive initial commercial payer coverage that reduced the cost associated with our patient co-pay assistance program. While final payer coverage decisions will continue to be made through this year and into 2023, gross to nets in the first half of the year have been better than anticipated.
Based on these trends and our expectations regarding payer coverage in the second half of the year, we are updating our expectations for gross to net adjustments for the full year to approximately 30%. Overall, we're increasing our full-year 2022 expectation for LYBALVI net sales from a range of $55 million-$75 million to a range of $75 million-$90 million. Moving on to our manufacturing and royalty business. In the second quarter, our manufacturing and royalty revenues were $85.3 million compared to $142.3 million in the prior year. The decrease was driven primarily by the previously disclosed J&J partial termination of the license agreement related to royalties from sales of the long-acting Invega products in the U.S.
We continue to disagree with J&J's actions, and in April, we initiated arbitration proceedings related to this matter. We continued to recognize royalty revenues from sales of the long-acting Invega products outside of the U.S. through the second quarter, as J&J has not terminated the agreement in these markets. Lastly, revenues from VUMERITY increased approximately 29% year-over-year to $26.2 million in the quarter. Turning now to expenses. Total operating expenses were $310.7 million for the second quarter, compared to $299.3 million in the same period in the prior year. This modest increase during a launch year reflects the operating leverage in the business and our continued focus on efficient allocation of capital.
For the second quarter, cost of goods sold increased approximately $5 million year-over-year to $58.4 million, driven primarily by higher volumes of key manufactured products. We've continued to prioritize our investments in R&D as we advance opportunities that may offer the highest potential return on investment. R&D expenses for the second quarter were $92.9 million, compared to $97.5 million for the same period in the prior year, reflecting focused investments as we advance nemvaleukin and our earlier stage neuroscience and oncology development programs, and as the required pediatric study for LYBALVI gets underway. SG&A expenses were $150.4 million compared to $139.2 million for the prior year, driven primarily by investments in the launch of LYBALVI.
Our top line results, combined with our continued focus on disciplined operating expense management, resulted in a GAAP net loss of $30.1 million and a non-GAAP net income of $10.5 million for the quarter. Turning to our balance sheet, we ended the second quarter in a strong financial position with approximately $760 million in cash and total investments and total debt outstanding of approximately $295 million, resulting in a positive net cash position of close to $465 million. I'll shift now to our financial expectations for 2022, which reflects strong operational performance in the first half of the year, notably with respect to the LYBALVI launch and updated assumptions around royalty revenues from ex-U.S. sales of the long-acting Invega products.
Our full expectations are outlined in the press release we issued earlier this morning. For the top line, we now expect higher total revenues in the range of $1.05 billion-$1.12 billion. A net increase of $40 million at the midpoint due to improved expectations for the LYBALVI launch and our updated assumption that we will continue to receive royalty revenues on ex-U.S. Sales of the long-acting Invega products through at least October 2022, reflecting the 3-month notice that Janssen would need to provide in order to terminate the license agreement in respect to these markets. We continue to believe that this is the most appropriate approach for financial planning purposes as we work through the arbitration process.
We expect these increases to be partially offset, primarily by lower anticipated VUMERITY manufacturing revenues driven by fewer commercial batches as we work with Biogen and one of its suppliers to address the potential supply constraints disclosed on Biogen's recent earnings call. Even as our top line has increased, we continue to actively manage our cost structure. Based on the anticipated timing of our investments and savings related to certain early-stage programs, we are reducing and narrowing our expectation for R&D expenses by approximately $10 million at the midpoint to a range of $380 million-$400 million. Our expectations for cost of goods sold and SG&A expenses remain unchanged. The strength of our top line and our continued disciplined expense management have driven improvements in our bottom line.
Our expectation for GAAP net loss has improved by $35 million at the midpoint, and our expectation for non-GAAP net income has improved by $45 million at the midpoint to a new range of $15 million-$45 million. Taking a step back, despite the current environment of inflationary pressures, constrained capital markets, and ongoing pandemic-related disruptions, we remain well-resourced and well-positioned to drive growth and execute against our strategic priorities. Even with a growing revenue base, efficient allocation of capital and management of our cost structure continue to be priorities for us and a virtue in the current volatile macroeconomic environment as we focus on driving shareholder value and long-term profitability. With that, I'll hand the call over to Todd to provide more detail on our commercial performance.
Thanks, Iain, and good morning, everyone. In the second quarter, total product revenue from our proprietary commercial portfolio grew approximately 19% year-over-year to $190.8 million. This portfolio is the engine behind our company's top-line performance. VIVITROL and ARISTADA performed well, and LYBALVI's strong launch uptake continued to validate the value proposition of this important medicine and to underscore the significant unmet need in the schizophrenia and bipolar I markets. I'll start with LYBALVI's performance during the quarter. Net sales were $20.1 million, reflecting robust unit growth. Total prescriptions in the second quarter were approximately 17,000, representing growth of approximately 64% quarter-over-quarter, driven by LYBALVI's differentiated product profile and our commercial execution. This strong demand was due in large part to increased prescriber breadth.
As of the end of the second quarter, approximately 4,260 prescribers had written a prescription for LYBALVI since its launch, which represents a 62% increase since the end of Q1. Based on our market research and anecdotal feedback from prescribers, interest in and experience with LYBALVI has grown within the treatment community. In a recent survey of 80 targeted healthcare providers, respondents cited both LYBALVI's overall efficacy and its weight gain profile compared to olanzapine in schizophrenia as a key driver of prescribing the product. Majority of the providers reported they intended to prescribe LYBALVI in the next 12 months. LYBALVI's utilization source of business in Q2 were consistent with the first quarter. Prescriptions were split evenly between schizophrenia and bipolar I patients, and patients switched to LYBALVI from olanzapine and other branded and generic agents.
This data underscores that prescribers consider LYBALVI as an appropriate option for a broad range of patients. LYBALVI's market access position continues to evolve as we engage in payer discussions and plans move through their formulary decision timelines. While this is underway, eligible patients have a pathway to access LYBALVI, supported by our patient and copay assistance programs. Broadly, as we expected, payer coverage decisions have been in line with other branded oral agents. We expect additional coverage decisions throughout the remainder of 2022 and into 2023. Taking a step back, with the year halfway complete and strong launch momentum, we are pleased to be raising our LYBALVI revenue expectations for 2022 based on strong underlying demand and prescriber adoption. We remain focused on executing our launch strategy and driving awareness of this important treatment option. Turning to ARISTADA.
For the ARISTADA product family, net sales in the second quarter increased to $74.6 million, driven primarily by TRx growth of 11% year-over-year on a month of therapy basis, outpacing the LAA market, which grew 7% year-over-year. We continue to focus on driving growth of this product family based on its differentiated profile and value proposition. We recently launched new digital marketing initiatives to drive awareness of ARISTADA and believe this will play an important role in expanding utilization going forward. VIVITROL net sales in the second quarter increased approximately 9% year-over-year to $96.1 million, driven primarily by the alcohol dependence indication. This indication accounted for approximately 60% of the VIVITROL business and has been the primary growth driver for the brand during the pandemic.
We expect this growth to continue as utilization for medication-assisted treatment increases in the alcohol dependence market. We also plan to continue to deploy resources to support awareness of VIVITROL as an important treatment option for opioid dependence. Our commercial results through the first half of the year are a reflection of the leverage in our commercial infrastructure, our sophisticated set of capabilities, and our unwavering commitment to execution. LYBALVI represents a significant opportunity for the company to drive shareholder value and have a meaningful impact on patients. LYBALVI, ARISTADA , and VIVITROL are distinctive products in their markets, and we are extremely proud to provide treatment options for people affected by serious mental illness and addiction. I look forward to updating you on our progress through the back half of the year. Now I'll turn the call over to Rich.
That's great. Thank you, Todd. We are managing the company based on three clear priorities. The first is our commercial business, growing revenues from our proprietary products with a focus on execution of the launch of LYBALVI. The second is executing our development plans for our oncology and neuroscience pipeline candidates to get to key decision points. The third is operating the business efficiently with a goal of driving long-term profitability. Midway through the year is a good time for us to assess our progress against these priorities. First, on the commercial business. As you've just heard from Todd, we continue to execute our commercial strategy across our psychiatry and addiction portfolio. VIVITROL and ARISTADA continue to grow and are important treatment options in their respective markets. With these two products, we operate in some of the most challenging disease areas and treatment systems in the pharmaceutical landscape.
Through our successes and challenges with these products, we've sharpened our commercial capabilities and established Alkermes as a trusted partner in serious mental illness and addiction. This is a strong foundation for LYBALVI. We've begun to establish a compelling launch trajectory and expect LYBALVI to be an important commercial asset for the long term. Our confidence is reinforced by the feedback we've received from physicians and patients using LYBALVI in the real-world setting. To see our design intention for LYBALVI realized in patients with schizophrenia and bipolar I is gratifying for everyone associated with this development and its launch. Our launch strategy and the investments we're making are reflective of and commensurate with the long-term opportunity, and we believe we're well positioned to deliver on the potential value of this important new medicine. Next, our R&D pipeline, starting with nemvaleukin alfa.
Nemvaleukin is now the most advanced IL-2 immunotherapy in the clinic. It is distinguished by its unique molecular design and the resulting pharmacology. The clinical responses we've seen, both as monotherapy and in combination, and the focused development strategy that we're pursuing. During the quarter, we presented data at ASCO from the ARTISTRY-1 study. As part of the presentation, we hosted oncology thought leaders who provided valuable clinical perspectives on the data, on nemvaleukin's differentiated attributes and its potential clinical utility, and on the importance of the IL-2 pathway in oncology. A replay of that discussion remains available on the investor section of our website. The data from ARTISTRY-1 established nemvaleukin's profile and our belief in its clinical potential, both as monotherapy and in combination with pembrolizumab in heavily pretreated patients across multiple tumor types.
The findings from ARTISTRY-1 informed our clinical development strategy, including the initiation of potential re-registration-enabling studies in two difficult-to-treat tumor types. ARTISTRY-6, evaluating nemvaleukin monotherapy in mucosal melanoma, and ARTISTRY-7, evaluating nemvaleukin in combination with pembrolizumab in platinum-resistant ovarian cancer. As we enter the second half of the year, we're focused on enrollment of these two studies. We'll also continue to enroll ARTISTRY-2 and ARTISTRY-3 to evaluate various dosing regimens, including once-weekly subQ dosing and less frequent IV dosing in a range of tumor types. Next is our orexin 2 receptor agonist program, ALKS-2680. In the first half of 2022, our priority was conducting IND-enabling activities as we prepare to enter a first-in-human study later this year. That work has progressed well, and we're on track to commence a single ascending dose study in the fourth quarter.
In the clinic, our goal is to answer critical questions early to enable data-driven decisions, and we plan to move quickly to conduct a proof-of-concept study in patients with narcolepsy next year. Turning to ALKS-1140, our selective HDAC inhibitor candidate. Consistent with our rigorous data-driven decision-making, we've decided to terminate ALKS-1140 clinical development program. As we disclosed earlier this year, initial data from the phase 1 dose-escalation study demonstrated higher than predicted levels of the major metabolite. Over the last several months, our team worked rapidly to generate additional data to establish the necessary exposure safety margins pre-clinically and characterize the profile of the metabolite to determine whether we should proceed to higher doses. The results of these efforts were clear and not supportive of a viable clinical candidate. We're currently evaluating the pharmaceutical properties of a number of backup molecules from the HDAC platform.
However, the threshold for advancing a new compound into the clinic will remain high. I'll end with our focus on managing the business efficiently with an emphasis on long-term profitability. The work we do as a developer of novel medicines is ambitious and can be extremely rewarding, but it's also inherently difficult and complex. Our focus on profitability and financial discipline provides a framework for making challenging and timely decisions. It requires that we continuously prioritize programs so that we invest in those that we believe offer the highest likelihood of success and return on investment. This rigorous allocation of capital is essential to running a biopharmaceutical company. Our portfolio of proprietary products drives our growth and profitability. As we execute the launch of LYBALVI, the operating leverage we've engineered into the business is becoming evident.
With the first half of the year now behind us, we're improving our financial expectations for both the top and bottom line for 2022. This is a result of our growth trajectory coupled with our cost management initiatives. To finish up, we are managing a dynamic business in a rapidly evolving macroeconomic landscape, and we're pleased with our execution year to date. We'll remain nimble as we execute on our strategic priorities in order to drive long-term profitability and deliver on our commitment to create value for our shareholders. With that, I'll turn the call to Sandy to manage the Q&A.
Thank you, Richard. Melissa, we'll now open the call for Q&A, please.
Thank you. If you'd like to ask a question, please press star one on your telephone keypad. A confirmation tone will indicate your line is in the question queue. You may press star two if you'd like to remove your question from the queue. For participants using speaker equipment, it may be necessary to pick up your handset before pressing the star keys. Our first question comes from the line of Brandon Folkes with Cantor Fitzgerald. Please proceed with your question.
Hi, thanks for taking my questions, and congratulations on a strong quarter. Two questions from me, both on LYBALVI. Pretty broad prescriber base to date. Can you just talk about what is perhaps needed to go deeper in this prescribing base of physicians? Is it really just time and experience with the product? Is it sort of rolling out coverage or just waiting for other patients to start cycling switches from other medications? Just any color there would be helpful. Then I'll ask my second question 'cause it may go together. Are you seeing LYBALVI move up in the treatment paradigm as yet, just either ahead of other brands or earlier on, when maybe a patient may have failed one or two generics, granted, you know, they always will have to fail generics? Thank you.
Yeah, I'll take both those questions. The first one around the breadth of prescribing, which we're really pleased with, month-over-month, quarter-over-quarter as well. What we've learned from our research and anecdotal feedback, we talked to a lot of our targeted physicians, non-targeted physicians, and what we've learned is that clinical experience with LYBALVI leads to a growing efficacy perceptions. Prescribers consistently report to us that the majority of their LYBALVI patients are doing well, and that they're expected to continue. Our belief right now is that the more experience that our targeted prescribers get with LYBALVI, they're seeing the value proposition play out, the efficacy of olanzapine, the weight mitigating benefits, very similar that was in our ENLIGHTEN-2 study. Our belief
I think that more clinical experience will drive growth, and we just think that's based just on timing. Our expectation Q3 and beyond is that prescriber breadth will continue to grow. In terms of positioning within lines of therapy, as you know, there are multiple lines of therapy. At this point, it's just too soon to tell. Our data is somewhat limited based on claims data regarding if LYBALVI has moved up. Our expectation, again, is that LYBALVI will be treated like a branded agent, which most branded agents are really utilized within the switch market. That's the place that LYBALVI will live.
Great. Thank you very much.
Thank you. Our next question comes from the line of Chris Shibutani with Goldman Sachs. Please proceed with your question.
Thank you very much, and congratulations on the LYBALVI trends and the raised guidance there. You commented that the utilization seems to be so far balanced between the schizophrenia and bipolar indications. Can you comment about whether you expect this to continue to be the case and how that's threaded into the balance of the year guidance? Also maybe talk about acute versus maintenance settings for each of those and what we might expect from a trend standpoint. Thank you.
Absolutely. Yeah, about half of LYBALVI patients thus far at this point in launch are schizophrenia patients, and approximately half are bipolar patients. We're also seeing that a fair amount are switches from olanzapine, which we did expect. You know, olanzapine is a meaningful product in the category. There are more olanzapine prescriptions written on an annual basis than the entire branded category. We know that's a very large switch opportunity. We know that physicians consistently report to us that two-thirds of olanzapine patients will gain weight, and that weight will happen within the first 8 weeks. We think there's a transition period that's very appropriate and opportunity for LYBALVI. Our expectation is that LYBALVI will be treated like other branded agent. We're seeing, again, a meaningful split between schizophrenia and bipolar.
I think it's important to remember that olanzapine currently holds approximately a 20% share in schizophrenia and about a 13% share in bipolar. They're both very large markets with meaningful opportunities. Our expectation is that split will continue. It could evolve a little bit over time, but we don't expect that will be in a meaningful way. At this point right now, when we look at the utilization, especially between acute and maintenance, we don't have data that actually speaks to because it's relatively early between acute and maintenance settings. I think it's important to remember that LYBALVI is a very broad indication. Schizophrenia, mixed episodes, maintenance episodes, monotherapy in bipolar, and also adjunctive therapy.
We really believe in the data starting to play out in anecdotal feedback that it's going to be used in a broad utility of settings and a broad utility of patients.
Thank you. Our next question comes from the line of Umer Raffat with Evercore ISI. Please proceed with your question.
Hi, guys. Thanks for taking my question. Just a couple, if I may. One, if the gross to net on LYBALVI is sort of stable quarter-over-quarter as per your disclosures, and the prescription data you report is around 17,000, which is about a 65% volume increase, that sort of implies, at least off of the 1Q run rate, reported sales closer to $22-$23 versus the $20 reported. I was just curious if there was any inventory or any other one-offs on the reported number you could speak to.
I guess the other one is, and again, there's lack of clarity on it, but I did notice you lowered the gross to net expectations from 40% to 30% for the full year, which does imply that the second half should track at sort of low- to mid-30s% on gross to net. Rich, I remember you made some comments at a recent broker conference suggesting you don't necessarily want to give up on gross to net early in the launch. I was just trying to square those two. Thank you very much.
Yes. Umer, I think in the prepared remarks earlier on, when we talked about the gross to net for LYBALVI, and sort of underlying demand is really what's driving the product at this point in time. The inventory level did increase during the quarter, by around $1.8 million, which is what we were expecting. As demand increases, you'd expect that inventory in the channel, would continue to increase as well. I wouldn't say there were anything unusual there. I think inventory is just tracking with the increase in demand.
More from a full year perspective, as we take the gross to net from 40% down to 30%, you know, I think pre-launch, we made a number of assumptions around various dynamics, things like channel mix, access, commercial contracting, and how much of the commercial business would be subject to NDC blocks. In reality, what we've seen is favorability on a number of fronts there, including lower rebating across all the channels and less full NDC block, with the latter, in particular, driving a lower cost associated with our co-pay assistance program. You're right that, you know, the gross to net average for the first half is around 26.5%.
To get to the 30, you'd see a tick up in the second half, and I think that would be more driven by sort of co-pay assistance utilization than anything else. But certainly not expecting that big step up in the second half of the year to get to anywhere near to 40%, which we'd originally talked to.
Thank you.
Thanks, Umer.
Thank you. Our next question comes from line of Akash Tewari with Jefferies. Please proceed with your question.
Hi, this is Amy on for Akash. Just two quick questions. The first one is, what type of healthy volunteer studies are you running for the OX2? Could these studies be longer than what Takeda ran in order to properly tease out the liver tox signal? On the VIVITROL IP, what's the impact of Teva's generic on the market? Would a potential entry force Alkermes to revisit its 2025 guidance? Thanks so much.
Hi, Amy, it's Rich. I'll take those. The first study that we're gonna run for the orexin program will be a single ascending dose in healthy volunteers. We'll probably run that outside the U.S. That study will be a traditional design of stepwise progression through ascending doses to get to what we expect to be either an MTD or a target engaging dose. From there, the only additional color we're gonna give today is that we're gonna move as quickly as we can into a proof of concept study in patients with narcolepsy as we clear those doses and move into the multiple dose study. Teva does not have a generic on the market yet. We're in a potential litigation with Teva now.
The latest update on that is that we expect a court date sometime in the fourth quarter. You know, obviously following that, we'll see how the business discussions or the legal process proceeds, but they're not on the market now. We're gonna. We've guided for 2022. We'll guide for 2023 in 2023, but we're, you know, we've always been optimistic about our IP position on VIVITROL. Even superseding all that is it's a very complicated market as you've heard over many years. It doesn't lend itself to a simple generic switching strategy.
Thank you. Our next question comes from the line of Cory Kasimov with J.P. Morgan. Please proceed with your question.
Hi, this is Tiffany on for Cory Kasimov. I'll add my congrats to the quarter. On LYBALVI, any changes in thinking about steady state gross to net given the better than expected payer coverage to date and then the lowered full year expectation? Any commentary on how you're thinking at this juncture about potential label expansion and their respective market opportunities for LYBALVI. Thanks.
Let me address the first one on LYBALVI steady-state gross to net. I think we're obviously pleased to be able to reduce the 2022 average rate from the 40% down to the 30%. I think as we go forward, it's gonna continue to be dynamic, you know, that initial 12-18 months post-launch, as we are achieving access across, you know, all the channels. I think steady-state's gonna be dependent largely upon what happens on the commercial contracting side of things. You know, we're not gonna comment specifically around our contracting strategy there, but that's gonna be a key determinant as to what the gross to net looks like longer term. There'll be more color on that as we proceed with the launch and into 2023.
In regards to lifecycle management, our focus right now is fulfilling our post-marketing commitments with the FDA. Iain mentioned in his prepared remarks, the pediatric study, which is a requirement, so we're focused on delivering against that as well. Outside of that, I think it's just important to remember that, you know, LYBALVI's in a very unique position right now. The brand actually launched with a very broad indication, schizophrenia and bipolar I disorder as well. That's a very unique position. Most products don't launch with such a broad indication. Our focus right now is maximizing those two indications, learning from our advisors in the field, and then over time, we'll make some decisions on what does the lifecycle management look like. That's into the future.
Right now, it's about. It's really around maximizing the current indications that we have.
Thank you.
Thank you. Our next question comes from the line of Paul Matteis with Stifel. Please proceed with your question.
Great. Thanks so much and congrats on the quarter and guidance raise. On LYBALVI, I wanted to just kinda understand a couple of the moving parts this quarter and the degree to which they were unexpected or not. The $1.8 million inventory build and the better than expected net price, was this embedded in your $18 million-$20 million guidance for the quarter, given that both of those aspects seem to be key in driving you reaching the top end of it? Then more broadly on the clinical context, I was curious, what are you seeing in terms of patients switching from olanzapine in terms of how long they've been on olanzapine previously? Are these patients who had been experiencing significant weight gain?
I understand every situation is different, but I'd be interested in some of the qualitative context as it just relates to when clinically patients are switching drugs onto LYBALVI. Thanks so much.
On the LYBALVI net sales dynamics, Paul, I'd say in the quarter, the increase in inventory was expected. We'd always thought that inventory levels would increase in line with demand. That was included into the 18%-20%. I would say the 26% gross to net, we did have favorability there as compared to what we originally thought. It's still a little bit of lower small numbers in so far as gross sales were $27 million in the quarter. One percentage point of gross to net, effectively $270,000. But there was a little bit of upside there on the gross to net side as compared to what we originally thought when we set the 18%-20%.
Yeah, in regards to the olanzapine dynamics as well, you know, the context is important. There's 7,000 patients that switch olanzapine treatment every single month.
It's a very broad amount of patients that switch. The data's been pretty consistent over the years in terms of the frequency. Claims data and physicians continue to report to us that the major driver of switching therapy is typically based upon tolerability with weight. We see that there's less tolerability for weight gain, especially for bipolar patients as well. It's something that we're watching pretty closely at this point. The switching opportunity at large is very big. You know, there's approximately 13,000 patients in a generic setting that switch to a branded agent. Again, there's about 7,000 olanzapine patients that switch. Over time, we're watching those dynamics very, very closely.
What we hear consistently and what we see, you know, at this early junction right now is that, you know, the major drivers of switching is really around efficacy. If physicians and patients have current or prior experience and a positive response to olanzapine, that's a good thing for LYBALVI. If they're experiencing weight issues or there's a lack of efficacy within the broader context of other generics or other branded agents, they will consider LYBALVI as well too. It's early days at this point, but we think that the switching dynamic, not only for olanzapine is strong, but also for the broader category is very large as well.
Great. Thank you for the color.
Thanks, Paul.
Thank you. Our next question comes from the line of Marc Goodman with SVB Leerink. Please proceed with your question.
Yes. Hi, just on LYBALVI gross to nets, I understand that you don't really wanna comment on kind of maintenance going forward, but I mean, if we started out thinking 40%, should we be thinking now, you know, 30%-35% kind of maintenance? I mean, can you at least give us some sense of. I mean, obviously the numbers have come down, so, you know, maybe you can just help us a little bit there. I may have missed this, but did you comment on persistence at all, or I just don't remember what you said, but I'd be curious there. On VUMERITY, is there anything else that you can tell us about where we are?
We understand there's a supply issue with the API, but I mean, is this something that's a major problem that you think is going to last all year, or is this something that you're fixing pretty quickly? Just curious on that. On the HDAC, I know you said that you're going to look at backup compounds. Are those far along? I'm just trying to remember. I think this came from an acquisition that you made, and there was a lead asset. I just don't remember, you know, what was behind it and whether this is something that we're gonna be waiting on for several years, or if you feel like, you know, you'll be back in the clinic, you know, kinda next year or, you know, with the new one. Thanks.
Marc, let me take the first one around the LYBALVI gross to net. I think originally we talked about steady state in that 35%-45%. The key driver is really gonna be what happens on the commercial contracting front, as we go through the remainder of this year and into 2023. You know, we don't wanna comment too specifically around what the contracting strategy is gonna be, from that perspective, but I think that range of 35%-45% is still valid. It's just where we're gonna end up within that range. And hi Marc, it's Todd. I'll take persistency questions as well. You know, the category at large is about five months. Our view right now is it's still a little early to really see what persistency would look like for LYBALVI.
No, we didn't comment on that. Over time, we'll be able to do that. We've got approximately 9,100 patients that have been on therapy. That number needs to grow for us to do, you know, the right type of analysis to really look at the persistency level. The best leading indicator that we have right now is what we hear from the marketplace, from physicians through our research as well. Prescribers report that the majority of their LYBALVI patients are doing well, and they are expecting them to continue on LYBALVI. We think that's a good leading indicator.
Mark, it's Rich. I'll take the last couple. On the VUMERITY side, I'll leave it to Biogen to give most of the updates on that. I'll just say to the extent that we're involved, our technical teams are highly involved, and we see a pathway to resolution of the manufacturing issues. Hopefully that will be resolved relatively quickly. On the HDACs, you're right. The original chemistry derived from the acquisition of Rodin a couple years ago. We have backups that come from that original chemistry that are quite well along the way. Then there might be some that are more remote because they're different structures. We're focused on the ones that derive from the original chemistry. We would...
I would say that we will move quickly on those over the next few months and make the call.
Thanks.
Thank you. Our next question comes from line of Douglas Tsao with H.C. Wainwright. Please proceed with your question.
Hi, good morning. Congrats on the progress. Rich, just given the fact that it seems like profitability is coming in a little ahead of plans with the raise in guidance, how are you thinking about the balance between potentially hitting some of the long-term financial targets in terms of margins versus perhaps investing a little bit more on some of the early-stage programs?
Yeah, I think we're deeply committed to hitting our long-term targets, and that's probably priority number one, just to show the financial discipline and reveal the growth and the leverage in the P&L. If we had additional capital to spend at this moment, I would probably emphasize it less on the early-stage compounds and more on LYBALVI right now as we see the momentum build for LYBALVI. You know, it's best to drill for oil in the fields that are already proven. I think ARISTADA, VIVITROL, and LYBALVI are growing nicely, and they have a lot of potential left in them, with an emphasis there on LYBALVI.
LYBALVI is our first real blockbuster potential drug as an oral compound in a large category, and the launch trajectory is just being established now, and that's what we wanna affect as much as we can in the near term.
Richard, as a follow-up, what specific investments would you make to drive some faster growth from LYBALVI?
DTC. That would be the focus in 2023 and beyond. That's the spend we'll probably titrate as we see access build over the next several months as well as the physician breadth. You really don't wanna turn on your DTC campaign if there are access restrictions or if a large number of physicians are unaware of your product. That's why you tend to wait a little bit later into the launch. It's all tracking to plan now, which is encouraging. Those are the triggers we'll pull as we move into 2023 and 2024.
Okay, great. I know people asked earlier in terms of LYBALVI on sort of lines of treatment, but I'm just curious, do you know how quickly from other drugs people are switching, sort of the weeks of therapy before making a switch to LYBALVI?
Yes, I'll take that one. The data that we watch very closely is just the dynamic on switching. Patients in schizophrenia and bipolar switch treatments on average about 5-7 times. Bipolar patients switch much more quickly. You know, directionally, you know, you're looking at a period of time of about 18-24 months, you'll see a bipolar patient switch pretty dramatically. A little bit longer for schizophrenia. Main reason for that is the bipolar patients don't tolerate issues with tolerability and/or efficacy as well too. That's why we think that LYBALVI has a really unique value proposition within that patient profile.
Okay, great. Thank you.
Thanks, Doug.
Thank you. Our next question comes from the line of Jason Gerberry, Bank of America. Please go ahead with your question.
Hi, good morning, everyone. This is Chi on for Jason. Thanks for taking our question. I guess I just have one on the IL-2 nemvaleukin. When can we expect an update on the alternative dosing with less frequent IV and subcut? Should we expect an update by year-end 2022? Would the update be a go, no-go decision, or would there be clinical data accompanying that update? I guess a follow-up to that would be now that, you know, sort of people have time to digest sort of the competitive update in the IL-2 front, specifically with the bempegaldesleukin updates, I'm curious, how has the strategic interest in this category has changed since then? Do you think what level of data do you think Alkermes would need to generate to sort of, you know, have that strategic interest?
Is it update from the alternative dosing, or do you think you need more clinical data to talk about efficacy of IL-2 in different tumor types? Thanks.
Hey, Chi, I'll take that. We're making good progress on both ARTISTRY-2 and ARTISTRY-3, ARTISTRY-2 being the once weekly subQ, ARTISTRY-3 being the less frequent IV. On the less frequent IV, it's actually a Bayesian design where we'll be looking at different doses and different regimens. We're quite confident that we'll come up with a less frequent IV dose, and the subQ has been underway for some time. We're seeing responses in the subQ. The question we're focused on subQ is durability. We wanna make sure that we have the same durability that characterizes IV IL-2. I would expect by the end of the year we'll have more insight. I'm not ready to make a call right now whether we'll make a go, no-go or whether we'll just have additional data.
Let's see how enrollment and durability persists over the year. We're well on our way in both of those. I do think that's an important component of assessing the commercial potential for IL-2 across multiple tumor types, understanding what the ultimate commercial dose might be. I think for a number of potential strategic partners, that's an important question. I think the most important part is of the discussions with folks is exactly what you referenced, letting the dust settle post bempegaldesleukin, which forces people to look at the IL-2s on an individual basis. In the case of nemvaleukin, thinking of it less as one of many IL-2 variants and more as a late-stage oncology product with its own data that support its value proposition. I think that's what's happening post ASCO.
That's why ASCO was so important for us to present all of the ARTISTRY-1 data so people could get a sense of this as an oncology agent, whether or not it's an IL-2 version at all. As I mentioned in the prepared remarks, nemvaleukin is now the most advanced IL-2 in development, and it's supported by a lot of not just efficacy data as monotherapy and in combination with pembrolizumab, but importantly, the design intention of this is to recapitulate the efficacy of high-dose IL-2 without the hallmark toxicities. The dataset is also augmented by a lot of safety data from a lot of patients that's helped confirm the design hypothesis.
You know, we'll keep going with ARTISTRY-6 and ARTISTRY-7, and we'll keep you know receptive to collaboration, and we'll collaborate when the time is right and the deal structure is appropriate for our shareholders.
Awesome. Great. Thanks.
Thank you. Ladies and gentlemen, there are no further questions at this time. I'll turn the floor back to the company for any final comments.
Thank you. Thanks everyone for joining us on the call this morning. Please don't hesitate to reach out to us at the company if you have any follow-up questions or if we can be otherwise helpful. Thanks so much. Have a great day.
Thank you. This concludes today's conference. You may disconnect your lines at this time. Thank you for your participation.